Frontiers in Pharmacology (Nov 2024)

Maslinic acid induces autophagy and ferroptosis via transcriptomic and metabolomic reprogramming in prostate cancer cells

  • Fen Hu,
  • Yuxi Sun,
  • Yunfeng Zhang,
  • Jiaxin Chen,
  • Yingzi Deng,
  • Yifei Li,
  • Ruobing Li,
  • Juan Zhang,
  • Yongping Liang,
  • Yan Liu,
  • Shuqing Wang,
  • Mi Li,
  • Lina Zhao,
  • Yuwei Liu,
  • Yuwei Liu,
  • Xiaodong Gong,
  • Xiaodong Gong,
  • Haifeng Cai,
  • Shouqin Gu,
  • Shouqin Gu

DOI
https://doi.org/10.3389/fphar.2024.1453447
Journal volume & issue
Vol. 15

Abstract

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Prostate cancer has the second highest incidence among male malignancies. Only a few studies exist on the inhibitory effects of maslinic acid (MA) on prostate cancer. Herein we found that MA inhibits prostate cancer cell proliferation by decreasing CDK2, CDK4, and CDK6 expression and concurrently increasing p27, Rb, p-Rb expression. Further, MA was observed to induce prostate cancer cell autophagy by increasing the expression of p53, p-p53, ULK1, Beclin1, Atg7, and Atg5 and the ratio of LC3-II/I and concurrently decreasing the expression of ERK1/2 and mTOR. In addition, MA induced RM-1 cell ferroptosis by regulating glutathione, glutamate, and oxidized glutathione concentrations, inhibiting SLC7A11 activity, and downregulating GPX4 expression. Integrated metabolome and transcriptome analysis led to the identification of key pathways (e.g., pathways in cancer and glutathione metabolism). Real-time quantitative PCR confirmed that MA regulates the expression of ABCA1, JUN, and NFKBIA. In vivo, we demonstrated that 50 mg/kg MA significantly inhibited the growth of tumors established using RM-1 cells. To summarize, we report that MA inhibits prostate cancer cell growth both in vitro and in vivo by inducing autophagy and ferroptosis via transcriptomic and metabolomic reprogramming.

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